Formulation, Characterization and in vitro Release of Topical Nanoemulsion Containing Prednisolone-Derived Corticosteroid

生物利用度 眼药水 药品 药理学 化学 Zeta电位 药物输送 色谱法 细胞毒性 皮质类固醇 体外 材料科学 纳米技术 医学 纳米颗粒 有机化学 生物化学 外科
作者
Sakine Tuncay Tanrıverdi,Evren Gökçe,Nilgün Öztürk,Mohammad Turk,Bita Entezari,Aylin Balcı,Ünnügülsüm Erdoğan,Emre Ozcanlar,Enis Işık,Banu Özkırım Arslan,Emre Erol Aldeniz,Udaya Kumar Dude,Özgen Özer
出处
期刊:Drug Development and Industrial Pharmacy [Taylor & Francis]
卷期号:: 1-19
标识
DOI:10.1080/03639045.2025.2455437
摘要

Prednisolone-Derived Corticosteroid (PDC), has anti-inflammatory activity in ocular administration. However, drug administration to the eye is extremely difficult due to the complex structure of the eye. Because of the ability of the eye to retain the drug and its physiology, the bioavailability of drugs applied to the eye is very low. One of the methods to overcome bioavailability problem is to formulate the drug as a nanoemulsion (NE). NEs are thermodynamically stable, colloidal drug delivery systems. They have small globule size and high surface area. These properties give them the ability to cross the biological membrane and increase the therapeutic efficacy of the drug molecule. The high energy method was used to create a NE eye drop formulation containing PDC, and the effects of changing homogenization processes on NE formation were investigated. After deciding on the optimum formulation; characterization, assay and in vitro release studies were performed, and the stability of the formulation was followed for 12 months. The optimum formulation selected initially had 126.6 ± 40.12nm and 99.9 ± 1.2% PDC, it had 125.4 ± 41.20nm and 99.29 ± 1.3% PDC after 12months in 25 °C 40%RH conditions. Cytotoxicity studies have shown no significant cytotoxic effects in NE containing PDC. The preparation and optimization of topical nanoemulsion formulations containing PDC for ocular inflammation treatment were achieved. The developed formulation was stable for 12months and no toxic effect was found in cell culture studies. This formulation could be useful as an alternative to PDC for ocular applications.

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